2007
DOI: 10.1021/jm061465o
|View full text |Cite
|
Sign up to set email alerts
|

Development of Novel Enkephalin Analogues that Have Enhanced Opioid Activities at Both μ and δ Opioid Receptors

Abstract: Enkephalin analogues with a 4-anilidopiperidine scaffold have been designed and synthesized to achieve therapeutic benefit for the treatment of pain due to mixed mu and delta opioid agonist activities. Ligand 16, in which a Dmt-substituted enkephalin-like structure was linked to the N-phenyl-N-piperidin-4-yl propionamide moiety, showed very high binding affinities (0.4 nM) at mu and delta receptors with an increased hydrophobicity (aLogP = 2.96). This novel lead compound was found to have very potent agonist a… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
2
2

Citation Types

1
25
0

Year Published

2009
2009
2024
2024

Publication Types

Select...
7
1

Relationship

2
6

Authors

Journals

citations
Cited by 40 publications
(26 citation statements)
references
References 23 publications
1
25
0
Order By: Relevance
“…Obtained compounds showed broad (47 nM to 76 μM) and μ-selective activities. For the synthesis of possible μ/δ compounds (Figure 19) amine ( 5 ) was coupled with protected phenylalanine or its p-F(Cl)-substituted analogs to give ( 123 ), which after deprotection were stepwise transferred to desired bivalent ligands ( 125 ) [193,194]. Compounds with X = H and D-Yyy-Ala showed potent binding affinities (0.4 nM) at μ and δreceptors with increased hydrophobicity (aLogP = 2.96), and potent agonist activities in the MVD (1.8 nM) and GPI (8.5 nM) assays [193].…”
Section: Bivalent Ligands Based On Fentanylmentioning
confidence: 99%
See 1 more Smart Citation
“…Obtained compounds showed broad (47 nM to 76 μM) and μ-selective activities. For the synthesis of possible μ/δ compounds (Figure 19) amine ( 5 ) was coupled with protected phenylalanine or its p-F(Cl)-substituted analogs to give ( 123 ), which after deprotection were stepwise transferred to desired bivalent ligands ( 125 ) [193,194]. Compounds with X = H and D-Yyy-Ala showed potent binding affinities (0.4 nM) at μ and δreceptors with increased hydrophobicity (aLogP = 2.96), and potent agonist activities in the MVD (1.8 nM) and GPI (8.5 nM) assays [193].…”
Section: Bivalent Ligands Based On Fentanylmentioning
confidence: 99%
“…For the synthesis of possible μ/δ compounds (Figure 19) amine ( 5 ) was coupled with protected phenylalanine or its p-F(Cl)-substituted analogs to give ( 123 ), which after deprotection were stepwise transferred to desired bivalent ligands ( 125 ) [193,194]. Compounds with X = H and D-Yyy-Ala showed potent binding affinities (0.4 nM) at μ and δreceptors with increased hydrophobicity (aLogP = 2.96), and potent agonist activities in the MVD (1.8 nM) and GPI (8.5 nM) assays [193]. Ligands with X = F, D-Yyy-Nle showed potent subnanomolar opioid agonist activity (IC 50 values of 0.37 and 0.26 nM in the MVD and GPI assays, respectively) with excellent efficacy (EC 50 = 0.07 nM, E max = 48% at hDOR; EC 50 = 0.29 nM, E max = 98% at rMOR) at both receptors.…”
Section: Bivalent Ligands Based On Fentanylmentioning
confidence: 99%
“…The co-administration of opioid agonists and a type of antidepressants, SSRIs, is expected to give a synergistic effect 17,18 and we herein set out to design an strategy to this co-administration, developing bifunctional ligands, an approach that has proven successful in the past for increasing potency and selectivity of many drugs. The drug design was based on bifunctional ligands interacting with two targets in a single molecule by combining two pharmacophores; opioid and SSRIs (Figure 1).…”
Section: Resultsmentioning
confidence: 99%
“…The SSRIs pharmacophore desmethylescitalopram 1 was combined with an opioid pharmacophore so that the designed ligands maintain the topographical structures of both pharmacophores, bearing in mind the development of previously designed μ-opioid selective 4-anilidopiperidine, and N -phenyl- N -piperidin-4-yl-propionamide analogues. 18 For the opioid agonist activity, enkephalin-like tetrapeptide structures (H-Tyr- D -Ala-Gly-Phe-) has been selected and modified. For the SSRIs activity, escitalopram, one of the most efficient SSRIs drug, has been selected and modified to get compound 1 .…”
Section: Resultsmentioning
confidence: 99%
“…enkephalin-analogs linked to a fentanyl unit (e.g. structure 3 )] 14,15. In specific cases, improved pharmacodynamic and pharmacokinetic properties like enhanced affinity, increased activity, relative to ‘the golden standard’ morphine, and high metabolic stability were observed 3,6.…”
mentioning
confidence: 99%